Abstract

Dietary lipid is important both quantitatively and qualitatively to human health, and intestinal processing of exogenous lipid is central to its assimilation. While much is known about luminal digestion of dietary lipid, its intracellular transport and processing are less well understood. These studies will focus on the two different fatty acid-binding proteins (FABPs) which are expressed in the enterocyte, intestinal-FABP and liver-FABP (IFABP and LFABP). While thought to be critical for enterocyte lipid trafficking, this has not been directly demonstrated. Nor is it clear why two homologous proteins that both bind FAs, are co-expressed in the enterocyte. Our earlier kinetics studies demonstrated marked differences between the proteins, suggesting that IFABP and LFABP are likely to have distinct functions We have now compared mice null for these FABPs for the first time, and the remarkable phenotypic differences observed indicate that they indeed have at least some unique roles, not only in enterocyte lipid metabolism, but even more so by leading to markedly different effects on whole body energy homeostasis. Specifically, we find that high fat-fed LFABP-/- mice are hyperphagic and markedly obese, yet do not display glucose intolerance and have improved exercise performance, thus displaying a metabolically healthy obese (MHO) phenotype. The IFABP-/- mouse is also healthier than WT, with improved glucose tolerance and more efficient intestinal lipid secretion. However in marked contrast to the LFABP-/-, the high fat-fed IFABP-/- mouse weighs less and accumulates less body fat and more lean mass than WT mice. Both null mice studied are global knockouts, and while IFABP is normally expressed only in intestine, LFABP is also highly expressed in liver, thus we do not yet know whether the dramatic changes in LFABP-/- mice are due to LFABP in intestine, liver, or both. It is also not yet known how loss of enterocyte IFABP leads to a lean phenotype. Interestingly, we have found changes in intestinal metabolism of fatty acids and monoacylglycerols and in levels of mucosal endocannabinoids (EC), in particular the MG 2-arachidonoyl glycerol, and hypothesize that these tissue-level effects of FABP ablation contribute, at least in part, to the whole body phenotypes. Based on these observations and questions, our aims are to 1) determine whether the hyperphagia and obesity observed in the LFABP-/- mouse are mediated via the EC system; 2) explore the mechanisms by which ablation of IFABP leads to decreased fat mass and body weight and increased lean body mass; 3) use our newly generated LFABP/IFABP double knockout mouse (L/I-DKO) to definitively determine whether the enterocyte FABPs are required for bulk lipid uptake; and 4) define the contributions of liver LFABP vs. intestinal FABP to the MHO LFABP-/- phenotype, and the contributions of intestinal FABPs (L + IFABP) vs. hepatic FABP (LFABP) to the downstream systemic effects of intestinal lipid processing. The proposed studies will use the L/I-DKO mouse, mice generated by conditional deletions of liver LFABP or intestinal LFABP, and adeno-associated viral replacement of LFABP vs. IFABP in the LFABP-/- and L/I-DKO liver, to provide important new information about enterocyte lipid transport and processing, and their relationships to systemic fuel metabolism.

Public Health Relevance

Lipid transport in the Intestine.Both the amount and type of dietary fat play an important role in uman health and disease. The uptake and transport of dietary fat by the small intestine is fundamental to how we assimilate this abundant source of calories in Western diets.While much is known about the digestion of dietary lipid in the gastrointestinal tract, far less is known about wha happens to diet derived lipid products within the intestinal mucosal cells themselves.Two different fatty acid bind ng proteins (FABP) are expressedin mucosa, liver type (LFABP) and intestinal type (IFABP). While they are proposed to be central to intestinal lipid uptake, it is not known why two separate FABP are present.Our previous studies suggested they may have unique functions, even though both proteins bind fatty acids. We have recently found that inhibition of LFABP leads to obesity, while inhibition of IFABP promotes leanness, supporting the idea of distinct functions. The proposed studies are aimed at understanding the individual roles of LFABP and IFABP in intracellular lipid transport, and in whole body fuel metabolism. The studies will primarily use genetically modified mice to examine these fundamental questions about how dietary lipids are processed by intestine, and sensed by the rest of the body.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK038389-29
Application #
9212802
Study Section
Integrative Nutrition and Metabolic Processes Study Section (INMP)
Program Officer
Perrin, Peter J
Project Start
1987-05-01
Project End
2020-01-31
Budget Start
2017-02-01
Budget End
2018-01-31
Support Year
29
Fiscal Year
2017
Total Cost
$352,717
Indirect Cost
$122,241

  Institution

Name
Rutgers University
Department
Nutrition
Type
Schools of Earth Sciences/Natur
DUNS #
001912864
City
Piscataway
State
NJ
Country
United States
Zip Code
08854

  Publications

Dasilva, Gabriel; Boller, Matthew; Medina, Isabel et al. (2018) Relative levels of dietary EPA and DHA impact gastric oxidation and essential fatty acid uptake. J Nutr Biochem 55:68-75
Onishi, Janet C; Campbell, Sara; Moreau, Michael et al. (2017) Bacterial communities in the small intestine respond differently to those in the caecum and colon in mice fed low- and high-fat diets. Microbiology 163:1189-1197
McCauliff, Leslie A; Storch, Judith (2017) Transport Assays for Sterol-Binding Proteins: Stopped-Flow Fluorescence Methods for Investigating Intracellular Cholesterol Transport Mechanisms of NPC2 Protein. Methods Mol Biol 1583:97-110
Wang, Qian; Rizk, Samar; Bernard, Cédric et al. (2017) Protocols and pitfalls in obtaining fatty acid-binding proteins for biophysical studies of ligand-protein and protein-protein interactions. Biochem Biophys Rep 10:318-324
McCauliff, Leslie A; Xu, Zhi; Li, Ran et al. (2015) Multiple Surface Regions on the Niemann-Pick C2 Protein Facilitate Intracellular Cholesterol Transport. J Biol Chem 290:27321-31
Douglass, John D; Zhou, Yin Xiu; Wu, Amy et al. (2015) Global deletion of MGL in mice delays lipid absorption and alters energy homeostasis and diet-induced obesity. J Lipid Res 56:1153-71
Gajda, Angela M; Storch, Judith (2015) Enterocyte fatty acid-binding proteins (FABPs): different functions of liver and intestinal FABPs in the intestine. Prostaglandins Leukot Essent Fatty Acids 93:9-16
Park, Woo-Jae; Park, Joo-Won; Merrill, Alfred H et al. (2014) Hepatic fatty acid uptake is regulated by the sphingolipid acyl chain length. Biochim Biophys Acta 1841:1754-66
Ilnytska, Olha; Santiana, Marianita; Hsu, Nai-Yun et al. (2013) Enteroviruses harness the cellular endocytic machinery to remodel the host cell cholesterol landscape for effective viral replication. Cell Host Microbe 14:281-93
Gajda, Angela M; Zhou, Yin Xiu; Agellon, Luis B et al. (2013) Direct comparison of mice null for liver or intestinal fatty acid-binding proteins reveals highly divergent phenotypic responses to high fat feeding. J Biol Chem 288:30330-44

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